Multi-omics analysis identifies therapeutic vulnerabilities in triple-negative breast cancer subtypes

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作者
Brian D. Lehmann
Antonio Colaprico
Tiago C. Silva
Jianjiao Chen
Hanbing An
Yuguang Ban
Hanchen Huang
Lily Wang
Jamaal L. James
Justin M. Balko
Paula I. Gonzalez-Ericsson
Melinda E. Sanders
Bing Zhang
Jennifer A. Pietenpol
X. Steven Chen
机构
[1] Vanderbilt University Medical Center,Department of Medicine
[2] Vanderbilt University Medical Center,Vanderbilt
[3] University of Miami Miller School of Medicine,Ingram Cancer Center
[4] University of Miami Miller School of Medicine,Department of Public Health Sciences
[5] Vanderbilt University Medical Center,Sylvester Comprehensive Cancer Center
[6] Vanderbilt University Medical Center,Department of Otolaryngology
[7] Baylor College of Medicine,Department of Pathology, Microbiology and Immunology
[8] Baylor College of Medicine,Lester and Sue Smith Breast Center
[9] Vanderbilt University,Department of Molecular and Human Genetics
来源
Nature Communications | / 12卷
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摘要
Triple-negative breast cancer (TNBC) is a collection of biologically diverse cancers characterized by distinct transcriptional patterns, biology, and immune composition. TNBCs subtypes include two basal-like (BL1, BL2), a mesenchymal (M) and a luminal androgen receptor (LAR) subtype. Through a comprehensive analysis of mutation, copy number, transcriptomic, epigenetic, proteomic, and phospho-proteomic patterns we describe the genomic landscape of TNBC subtypes. Mesenchymal subtype tumors display high mutation loads, genomic instability, absence of immune cells, low PD-L1 expression, decreased global DNA methylation, and transcriptional repression of antigen presentation genes. We demonstrate that major histocompatibility complex I (MHC-I) is transcriptionally suppressed by H3K27me3 modifications by the polycomb repressor complex 2 (PRC2). Pharmacological inhibition of PRC2 subunits EZH2 or EED restores MHC-I expression and enhances chemotherapy efficacy in murine tumor models, providing a rationale for using PRC2 inhibitors in PD-L1 negative mesenchymal tumors. Subtype-specific differences in immune cell composition and differential genetic/pharmacological vulnerabilities suggest additional treatment strategies for TNBC.
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